Impact drugs targeting cardiometabolic risk on the gut microbiota

Manon Balvers; Bert-Jan H. van den Born; Evgeni Levin; Max Nieuwdorp

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Impact drugs targeting cardiometabolic risk on the gut microbiota

机译：靶向肠道微生物植物的心细素风险的影响药物

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Purpose of review Alterations in the gut microbiome composition or function are associated with risk factors for cardiometabolic diseases, including hypertension, hyperlipidemia and hyperglycemia. Based on recent evidence that also oral medications used to treat these conditions could alter the gut microbiome composition and function and, vice versa, that the gut microbiome could affect the efficacy of these treatments, we reviewed the literature on these observed interactions. Recent findings While the interaction of metformin with the gut microbiome has been studied most, other drugs that target cardiometabolic risk are gaining attention and often showed associations with alterations in microbiome-related features, including alterations in specific microbial taxa or pathways, microbiome composition or microbiome-derived metabolites, while the gut microbiome was also involved in drug metabolism and drug efficacy. As for metformin, for some of them even a potential therapeutic effect via the gut microbiome is postulated. However, exact mechanisms remain to be elucidated. Summary There is growing interest in clarifying the interactions between the gut microbiome and drugs to treat hypertension, hyperlipidemia and hyperglycemia as well as the first pass effect of microbiome on drug efficacy. While mostly analysed in animal models, also human studies are gaining more and more traction. Improving the understanding of the gut microbiome drug interaction can provide clinical directions for therapy by optimizing drug efficacy or providing new targets for drug development.

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《Current opinion in lipidology》 |2021年第1期|共17页
作者
Manon Balvers; Bert-Jan H. van den Born; Evgeni Levin; Max Nieuwdorp;
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作者单位

Department of Internal and Vascular Medicine Amsterdam UMC Location AMC University of Amsterdam;

Department of Internal and Vascular Medicine Amsterdam UMC Location AMC University of Amsterdam;

Department of Internal and Vascular Medicine Amsterdam UMC Location AMC University of Amsterdam;

Department of Internal and Vascular Medicine Amsterdam UMC Location AMC University of Amsterdam;

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原文格式 PDF
正文语种 eng
中图分类生物化学;
关键词
antihyperglycemic drugs; antihyperlipidemic drugs; antihypertensive drugs; drug; microbiome;

机译：抗血糖药物;抗高血病药物;抗高血压药物;药物;微生物组;

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4. Targeted inhibition of gut microbiota proteins involved in TMAO production to reduce platelet aggregation and arterial thrombosis: a blueprint for drugging the microbiota in the treatment of cardiometabolic disease? [J] . van Mens T. E., Buller H. R., Nieuwdorp M. Journal of thrombosis and haemostasis: JTH . 2019,第1期

机译：针对肠道微生物蛋白的靶向抑制，参与TMAO生产以减少血小板聚集和动脉血栓形成：用于在治疗心细素疾病的微生物群中吸毒的蓝图？
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机译：同居与肠道菌群更大的相似性有关这可能会影响心脏代谢和炎症风险
10. Targeted inhibition of gut microbiota proteins involved in TMAO production to reduce platelet aggregation and arterial thrombosis: a blueprint for drugging the microbiota in the treatment of cardiometabolic disease? [O] . T. E. Mens, H. R. Büller, M. Nieuwdorp 2018

机译：针对肠道微生物蛋白的靶向抑制参与TMAO生产以减少血小板聚集和动脉血栓形成：用于在治疗心细素疾病的微生物群中吸毒的蓝图？
11. Role of Bactericidal Peptidoglycan Recognition Proteins in Regulating Gut Microbiota and Obesity. [R] . Gupta, D. 2018

机译：杀菌肽聚糖识别蛋白在调节肠道微生物和肥胖中的作用。

Impact drugs targeting cardiometabolic risk on the gut microbiota

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